Li D, Tapscoft T, Gonzalez O, Burch P E, Quiñones M A, Zoghbi W A, Hill R, Bachinski L L, Mann D L, Roberts R
Section of Cardiology, Molecular Biology Computational Resource, Baylor College of Medicine, Houston, TX, USA.
Circulation. 1999 Aug 3;100(5):461-4. doi: 10.1161/01.cir.100.5.461.
Idiopathic dilated cardiomyopathy, of which approximately 20% of cases are familial (FDCM), is a primary myocardial disorder characterized by ventricular dilatation and impaired systolic function. It is a common cause of heart failure and the need for cardiac transplantation. Although 6 chromosomal loci responsible for autosomal dominant FDCM have been mapped by linkage analysis, none of these genes have been identified. By use of the candidate-gene approach, actin was identified recently as being responsible for dilated cardiomyopathy. Considerable evidence suggests desmin, a muscle-specific intermediate filament, plays a significant role in cardiac growth and development.
To determine whether a defect of desmin induces dilated cardiomyopathy, 44 probands with FDCM underwent clinical evaluation and DNA analysis. Diagnostic criteria, detected by echocardiography, consisted of ventricular dimension of >/=2.7 cm/m(2) with an ejection fraction </=50% in the absence of other potential causes. After amplification by polymerase chain reaction, the exons of the desmin gene were sequenced. A missense desmin mutation, Ile451Met, which cosegregates with FDCM without clinically evident skeletal muscle abnormalities, was identified in a 4-generation family but was not detected in 460 unrelated healthy individuals.
A novel missense mutation of desmin, Ile451Met, was identified as the genetic cause of idiopathic dilated cardiomyopathy. This finding is of particular significance because this is the first mutation detected in the desmin tail domain, and the function of the desmin tail remains unknown. Because this mutation leads to a restricted cardiac phenotype in the family studied in the present report, it suggests that the tail of desmin plays an important functional role in cardiac tissue.
特发性扩张型心肌病,约20%的病例为家族性(家族性扩张型心肌病,FDCM),是一种以心室扩张和收缩功能受损为特征的原发性心肌疾病。它是心力衰竭和心脏移植需求的常见原因。尽管通过连锁分析已定位了6个与常染色体显性遗传FDCM相关的染色体位点,但这些基因均未被鉴定出来。最近通过候选基因方法,已确定肌动蛋白是导致扩张型心肌病的原因。大量证据表明,结蛋白作为一种肌肉特异性中间丝,在心脏生长和发育中起重要作用。
为确定结蛋白缺陷是否会导致扩张型心肌病,对44例FDCM先证者进行了临床评估和DNA分析。通过超声心动图检测的诊断标准包括:在无其他潜在病因的情况下,心室维度≥2.7 cm/m²且射血分数≤50%。经聚合酶链反应扩增后,对结蛋白基因的外显子进行测序。在一个四代家族中发现了一个错义结蛋白突变Ile451Met,它与FDCM共分离且无明显的临床骨骼肌异常,但在460名无关健康个体中未检测到。
一种新的结蛋白错义突变Ile451Met被确定为特发性扩张型心肌病的遗传病因。这一发现具有特别重要的意义,因为这是在结蛋白尾部结构域检测到的首个突变,且结蛋白尾部的功能仍不清楚。由于该突变在本报告研究的家族中导致了局限于心脏的表型,这表明结蛋白尾部在心脏组织中发挥着重要的功能作用。
